Thimerosal Induces Apoptosis in a Neuroblastoma Model Via the cJun N-Terminal Kinase Pathway

doi:10.1093/toxsci/kfj205

ToxSci Advance Access published online on April 19, 2006
Toxicological Sciences, doi:10.1093/toxsci/kfj205

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© The Author 2006. Published by Oxford University Press on behalf of the Society of Toxicology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org
Received January 9, 2006
Accepted April 17, 2006

Neurotoxicology

Thimerosal Induces Apoptosis in a Neuroblastoma Model Via the cJun N-Terminal Kinase Pathway

Michelle L. Herdman ¹, Aileen Marcelo ¹, Ying Huang ², Richard M. Niles ², Sanjit Dhar ³, and Kinsley K. Kiningham ¹ ^*

¹ Departments of Pharmacology, Physiology, and Toxicology, Joan C. Edwards School of Medicine, Marshall University, Huntington, WV 25704
² Departments of Biochemistry and Microbiology, Joan C. Edwards School of Medicine, Marshall University, Huntington, WV 25704
³ University of Kentucky, Lexington, KY 40536

^* To whom correspondence should be addressed.
Kinsley K. Kiningham, E-mail: Kiningham{at}marshall.edu

Abstract

The cJun N-terminal kinase (JNK) signaling pathway is activatedin response to a variety of stimuli, including environmentalinsults, and has been implicated in neuronal apoptosis. In thisstudy, we investigated the role that the JNK pathway plays inneurotoxicity caused by thimerosal, an ethylmercury-containingpreservative. SK-N-SH cells treated with thimerosal (0-10 µM)showed an increase in the phosphorylated (active) form of JNKand cJun with 5 and 10 µM thimerosal treatment at 2 and4 h. To examine Activator Protein-1 (AP-1) transcription, cellswere transfected with a pGL2 vector containing four AP-1 consensussequences and then treated with thimerosal (0-2.5 µM) for24 h. Luciferase studies showed an increase in AP-1 transcriptionalactivity upon thimerosal administration. To determine the componentsof the AP-1 complex, cells were transfected with either a dominantnegative to cFos (A-Fos) or cJun (TAM67). Reporter analysisshowed that TAM67, but not A-Fos, decreased AP-1 transcriptionalactivity, indicating a role for cJun in this pathway. To assesswhich components are essential to apoptosis, cells were treatedwith a cell-permeable JNK inhibitor II (SP600125) or transfectedwith TAM67, and downstream effectors of apoptosis were analyzed.Cells pretreated with SP600125 showed decreases in activationof caspase 9 and 3, decreases in degradation of poly(ADP-ribose)polymerase (PARP), and decreased levels of pro-apoptotic Bim,in comparison to cells treated with thimerosal alone. However,cells transfected with TAM67 showed no changes in those samecomponents. Taken together, these results indicate that thimerosal-inducedneurotoxicity occurs through the JNK signaling pathway, independentof cJun activation, leading ultimately to apoptotic cell death.

Keywords: thimerosal; mercury; neurotoxicity; JNK; cJun; Bim.

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